Elucidation of MRAS-mediated Noonan syndrome with cardiac hypertrophy
Erin M. Higgins, … , Raul Urrutia, Michael J. Ackerman
Erin M. Higgins, … , Raul Urrutia, Michael J. Ackerman
Published March 9, 2017
Citation Information: JCI Insight. 2017;2(5):e91225. https://doi.org/10.1172/jci.insight.91225.
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Research Article Cardiology Genetics

Elucidation of MRAS-mediated Noonan syndrome with cardiac hypertrophy

Abstract

Noonan syndrome (NS; MIM 163950) is an autosomal dominant disorder and a member of a family of developmental disorders termed “RASopathies,” which are caused mainly by gain-of-function mutations in genes encoding RAS/MAPK signaling pathway proteins. Whole exome sequencing (WES) and trio-based genomic triangulation of a 15-year-old female with a clinical diagnosis of NS and concomitant cardiac hypertrophy and her unaffected parents identified a de novo variant in MRAS-encoded RAS-related protein 3 as the cause of her disease. Mutation analysis using in silico mutation prediction tools and molecular dynamics simulations predicted the identified variant, p.Gly23Val-MRAS, to be damaging to normal protein function and adversely affect effector interaction regions and the GTP-binding site. Subsequent ectopic expression experiments revealed a 40-fold increase in MRAS activation for p.Gly23Val-MRAS compared with WT-MRAS. Additional biochemical assays demonstrated enhanced activation of both RAS/MAPK pathway signaling and downstream gene expression in cells expressing p.Gly23Val-MRAS. Mutational analysis of MRAS in a cohort of 109 unrelated patients with phenotype-positive/genotype-negative NS and cardiac hypertrophy yielded another patient with a sporadic de novo MRAS variant (p.Thr68Ile, c.203C>T). Herein, we describe the discovery of mutations in MRAS in patients with NS and cardiac hypertrophy, establishing MRAS as the newest NS with cardiac hypertrophy-susceptibility gene.

Authors

Erin M. Higgins, J. Martijn Bos, Heather Mason-Suares, David J. Tester, Jaeger P. Ackerman, Calum A. MacRae, Katia Sol-Church, Karen W. Gripp, Raul Urrutia, Michael J. Ackerman

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Figure 3

Root-mean-square deviation and root-mean-square fluctuation values of both WT-MRAS and p.Gly23Val-MRAS during the molecular dynamic simulations.

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Root-mean-square deviation and root-mean-square fluctuation values of bo...
(A and B) Root-mean-square deviation (RMSD) values for WT-MRAS (A) and p.Gly23Val-MRAS (B). (C and D) Root-mean-square fluctuation (RMSF) values for WT-MRAS (C) and p.Gly23Val-MRAS (D) are used here as a measure of the flexibility of different regions of the protein during the 20-ns molecular dynamic simulations (MDS). The black boxes represent the switch I region and the blue boxes represent the switch II region. The dynamics of these regions are critical for the transition from state I to state II.